Brd4 is on the move during inflammation

被引:37
作者
Xu, Yali [1 ,2 ]
Vakoc, Christopher R. [1 ]
机构
[1] Cold Spring Harbor Lab, Cold Spring Harbor, NY 11724 USA
[2] SUNY Stony Brook, Mol & Cellular Biol Program, Stony Brook, NY 11794 USA
来源
TRENDS IN CELL BIOLOGY | 2014年 / 24卷 / 11期
基金
英国惠康基金;
关键词
Brd4; p65; NF-kappa B; enhancer; super-enhancer; inflammation; JQl; BET bromodomain; TRANSCRIPTION FACTORS; MACROPHAGE; ENHANCERS; CELLS;
D O I
10.1016/j.tcb.2014.09.005
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Enhancer landscapes are shaped by the integrated functions of lineage-specific and signal-dependent transcription factors. A new study by Brown et al. suggests that the signal-dependent transcription factor NF-kappa B can modulate global enhancer activities by altering the occupancy of Brd4, a BET bromodomain coactivator protein, across the genome. This work reveals new principles of enhancer dynamics and insights into the therapeutic modulation of enhancer function with BET bromodomain inhibitors.
引用
收藏
页码:615 / 616
页数:2
相关论文
共 10 条
[1]  
Brown JD, 2014, MOL CELL
[2]   Simple Combinations of Lineage-Determining Transcription Factors Prime cis-Regulatory Elements Required for Macrophage and B Cell Identities [J].
Heinz, Sven ;
Benner, Christopher ;
Spann, Nathanael ;
Bertolino, Eric ;
Lin, Yin C. ;
Laslo, Peter ;
Cheng, Jason X. ;
Murre, Cornelis ;
Singh, Harinder ;
Glass, Christopher K. .
MOLECULAR CELL, 2010, 38 (04) :576-589
[3]   Brd4 Coactivates Transcriptional Activation of NF-κB via Specific Binding to Acetylated RelA [J].
Huang, Bo ;
Yang, Xiao-Dong ;
Zhou, Ming-Ming ;
Ozato, Keiko ;
Chen, Lin-Feng .
MOLECULAR AND CELLULAR BIOLOGY, 2009, 29 (05) :1375-1387
[4]   A high-resolution map of the three-dimensional chromatin interactome in human cells [J].
Jin, Fulai ;
Li, Yan ;
Dixon, Jesse R. ;
Selvaraj, Siddarth ;
Ye, Zhen ;
Lee, Ah Young ;
Yen, Chia-An ;
Schmitt, Anthony D. ;
Espinoza, Celso A. ;
Ren, Bing .
NATURE, 2013, 503 (7475) :290-294
[5]   Remodeling of the Enhancer Landscape during Macrophage Activation Is Coupled to Enhancer Transcription [J].
Kaikkonen, Minna U. ;
Spann, Nathanael J. ;
Heinz, Sven ;
Romanoski, Casey E. ;
Allison, Karmel A. ;
Stender, Joshua D. ;
Chun, Hyun B. ;
Tough, David F. ;
Prinjha, Rab K. ;
Benner, Christopher ;
Glass, Christopher K. .
MOLECULAR CELL, 2013, 51 (03) :310-325
[6]   Selective Inhibition of Tumor Oncogenes by Disruption of Super-Enhancers [J].
Loven, Jakob ;
Hoke, Heather A. ;
Lin, Charles Y. ;
Lau, Ashley ;
Orlando, David A. ;
Vakoc, Christopher R. ;
Bradner, James E. ;
Lee, Tong Ihn ;
Young, Richard A. .
CELL, 2013, 153 (02) :320-334
[7]   Suppression of inflammation by a synthetic histone mimic [J].
Nicodeme, Edwige ;
Jeffrey, Kate L. ;
Schaefer, Uwe ;
Beinke, Soren ;
Dewell, Scott ;
Chung, Chun-wa ;
Chandwani, Rohit ;
Marazzi, Ivan ;
Wilson, Paul ;
Coste, Herve ;
White, Julia ;
Kirilovsky, Jorge ;
Rice, Charles M. ;
Lora, Jose M. ;
Prinjha, Rab K. ;
Lee, Kevin ;
Tarakhovsky, Alexander .
NATURE, 2010, 468 (7327) :1119-1123
[8]   Latent Enhancers Activated by Stimulation in Differentiated Cells [J].
Ostuni, Renato ;
Piccolo, Viviana ;
Barozzi, Iros ;
Polletti, Sara ;
Termanini, Alberto ;
Bonifacio, Silvia ;
Curina, Alessia ;
Prosperini, Elena ;
Ghisletti, Serena ;
Natoli, Gioacchino .
CELL, 2013, 152 (1-2) :157-171
[9]   Enhancer biology and enhanceropathies [J].
Smith, Edwin ;
Shilatifard, Ali .
NATURE STRUCTURAL & MOLECULAR BIOLOGY, 2014, 21 (03) :210-219
[10]   Transcription factors: from enhancer binding to developmental control [J].
Spitz, Francois ;
Furlong, Eileen E. M. .
NATURE REVIEWS GENETICS, 2012, 13 (09) :613-626
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